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同源κ-神经毒素与烟碱型乙酰胆碱受体的α3亚基存在残基特异性相互作用:κ-银环蛇毒素和κ-黄腹海蛇毒素结合的结构要求比较。

Homologous kappa-neurotoxins exhibit residue-specific interactions with the alpha 3 subunit of the nicotinic acetylcholine receptor: a comparison of the structural requirements for kappa-bungarotoxin and kappa-flavitoxin binding.

作者信息

McLane K E, Weaver W R, Lei S, Chiappinelli V A, Conti-Tronconi B M

机构信息

Department of Biochemistry, University of Minnesota, St. Paul 55108.

出版信息

Biochemistry. 1993 Jul 13;32(27):6988-94. doi: 10.1021/bi00078a025.

DOI:10.1021/bi00078a025
PMID:8334127
Abstract

kappa-Flavotoxin (kappa-FTX), a snake neurotoxin that is a selective antagonist of certain neuronal nicotinic acetylcholine receptors (AChRs), has recently been isolated and characterized [Grant, G. A., Frazier, M. W., & Chiappinelli, V. A. (1988) Biochemistry 27, 1532-1537]. Like the related snake toxin kappa-bungarotoxin (kappa-BTX), kappa-FTX binds with high affinity to alpha 3 subtypes of neuronal AChRs, even though there are distinct sequence differences between the two toxins. To further characterize the sequence regions of the neuronal AChR alpha 3 subunit involved in formation of the binding site for this family of kappa-neurotoxins, we investigated kappa-FTX binding to overlapping synthetic peptides screening the alpha 3 subunit sequence. A sequence region forming a "prototope" for kappa-FTX was identified within residues alpha 3 (51-70), confirming the suggestions of previous studies on the binding of kappa-BTX to the alpha 3 subunit [McLane, K. E., Tang, F., & Conti-Tronconi, B. M. (1990) J. Biol. Chem. 265, 1537-1544] and alpha-bungarotoxin to the Torpedo AChR alpha subunit [Conti-Tronconi, B. M., Tang, F., Diethelm, B. M., Spencer, S. R., Reinhardt-Maelicke, S., & Maelicke, A. (1990) Biochemistry 29, 6221-6230] that this sequence region is involved in formation of a cholinergic site. Single residue substituted analogues, where each residue of the sequence alpha 3 (51-70) was sequentially replaced by a glycine, were used to identify the amino acid side chains involved in the interaction of this prototope with kappa-FTX.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

κ-黄曲霉毒素(κ-FTX)是一种蛇神经毒素,是某些神经元烟碱型乙酰胆碱受体(AChRs)的选择性拮抗剂,最近已被分离和鉴定[格兰特,G.A.,弗雷泽,M.W.,& 基亚皮内利,V.A.(1988年)《生物化学》27卷,第1532 - 1537页]。与相关的蛇毒素κ-银环蛇毒素(κ-BTX)一样,κ-FTX与神经元AChRs的α3亚型具有高亲和力结合,尽管这两种毒素之间存在明显的序列差异。为了进一步表征神经元AChRα3亚基中参与该家族κ-神经毒素结合位点形成的序列区域,我们研究了κ-FTX与筛选α3亚基序列的重叠合成肽的结合情况。在α3(51 - 70)残基内鉴定出一个形成κ-FTX“原表位”的序列区域,证实了先前关于κ-BTX与α3亚基结合的研究[麦克莱恩,K.E.,唐,F.,& 孔蒂 - 特龙科尼,B.M.(1990年)《生物化学杂志》265卷,第1537 - 1544页]以及α-银环蛇毒素与电鳐AChRα亚基结合的研究[孔蒂 - 特龙科尼,B.M.,唐,F.,迪特尔姆,B.M.,斯宾塞,S.R.,莱因哈特 - 迈利克,S.,& 迈利克,A.(1990年)《生物化学》29卷,第6221 - 6230页]的推测,即该序列区域参与胆碱能位点的形成。使用单残基取代类似物,其中α3(51 - 70)序列中的每个残基依次被甘氨酸取代,以鉴定该原表位与κ-FTX相互作用中涉及的氨基酸侧链。(摘要截断于250字)

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